Brucella abortus LPS inhibitors belong to a specific class of chemical compounds that have garnered attention in the field of microbiology and immunology. Brucella abortus is a gram-negative bacterium known for causing brucellosis, a zoonotic infectious disease that primarily affects livestock, including cattle, goats, and sheep, but can also infect humans. The bacterium's lipopolysaccharide (LPS) is a critical component of its outer membrane and is involved in various aspects of host-pathogen interactions, including immune evasion and modulation. LPS inhibitors targeting Brucella abortus aim to interfere with the structure, function, or recognition of the bacterium's LPS, potentially affecting its virulence and interactions with the host immune system.
The mechanism of action of Brucella abortus LPS inhibitors typically involves their binding to specific sites or domains within the LPS molecule or enzymes involved in LPS biosynthesis. This interaction can lead to changes in the LPS structure or modification patterns, potentially impacting the bacterium's ability to evade host immune responses or maintain membrane integrity. Consequently, Brucella abortus LPS inhibitors may have implications for the study of Brucella pathogenesis and immune evasion mechanisms, offering insights into the molecular mechanisms that govern the host-pathogen interactions during brucellosis. Their development is instrumental in advancing our understanding of bacterial infections, providing valuable tools for investigating the roles of LPS in Brucella abortus virulence and host responses to infection.
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Product Name | CAS # | Catalog # | QUANTITY | Price | Citations | RATING |
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D-Cycloserine | 68-41-7 | sc-221470 sc-221470A sc-221470B sc-221470C | 200 mg 1 g 5 g 25 g | $27.00 $75.00 $139.00 $520.00 | 4 | |
Inhibits cell wall synthesis in bacteria, which may indirectly reduce the expression of LPS in Brucella abortus. |